292 resultados para Dell, Richard
Resumo:
Prehension in an act of coordinated reaching and grasping. The reaching component is concerned with bringing the hand to object to be grasped (transport phase); the grasping component refers to the shaping of the hand according to the object features (grasping phase) (Jeannerod, 1981). Reaching and grasping involve different muscles, proximal and distal muscles respectively, and are controlled by different parietofrontal circuit (Jeannerod et al., 1995): a medial circuit, involving area of superior parietal lobule and dorsal premotor area 6 (PMd) (dorsomedial visual stream), is mainly concerned with reaching; a lateral circuit, involving the inferior parietal lobule and ventral premotor area 6 (PMv) (dorsolateral visual stream), with grasping. Area V6A is located in the caudalmost part of the superior parietal lobule, so it belongs to the dorsomedial visual stream; it contains neurons sensitive to visual stimuli (Galletti et al. 1993, 1996, 1999) as well as cells sensitive to the direction of gaze (Galletti et al. 1995) and cells showing saccade-related activity (Nakamura et al. 1999; Kutz et al. 2003). Area V6A contains also arm-reaching neurons likely involved in the control of the direction of the arm during movements towards objects in the peripersonal space (Galletti et al. 1997; Fattori et al. 2001). The present results confirm this finding and demonstrate that during the reach-to-grasp the V6A neurons are also modulated by the orientation of the wrist. Experiments were approved by the Bioethical Committee of the University of Bologna and were performed in accordance with National laws on care and use of laboratory animals and with the European Communities Council Directive of 24th November 1986 (86/609/EEC), recently revised by the Council of Europe guidelines (Appendix A of Convention ETS 123). Experiments were performed in two awake Macaca fascicularis. Each monkey was trained to sit in a primate chair with the head restrained to perform reaching and grasping arm movements in complete darkness while gazing a small fixation point. The object to be grasped was a handle that could have different orientation. We recorded neural activity from 163 neurons of the anterior parietal sulcus; 116/163 (71%) neurons were modulated by the reach-to-grasp task during the execution of the forward movements toward the target (epoch MOV), 111/163 (68%) during the pulling of the handle (epoch HOLD) and 102/163 during the execution of backward movements (epoch M2) (t_test, p ≤ 0.05). About the 45% of the tested cells turned out to be sensitive to the orientation of the handle (one way ANOVA, p ≤ 0.05). To study how the distal components of the movement, such as the hand preshaping during the reaching of the handle, could influence the neuronal discharge, we compared the neuronal activity during the reaching movements towards the same spatial location in reach-to-point and reach-to-grasp tasks. Both tasks required proximal arm movements; only the reach-to-grasp task required distal movements to orient the wrist and to shape the hand to grasp the handle. The 56% of V6A cells showed significant differences in the neural discharge (one way ANOVA, p ≤ 0.05) between the reach-to-point and the reach-to-grasp tasks during MOV, 54% during HOLD and 52% during M2. These data show that reaching and grasping are processed by the same population of neurons, providing evidence that the coordination of reaching and grasping takes place much earlier than previously thought, i.e., in the parieto-occipital cortex. The data here reported are in agreement with results of lesions to the medial posterior parietal cortex in both monkeys and humans, and with recent imaging data in humans, all of them indicating a functional coupling in the control of reaching and grasping by the medial parietofrontal circuit.
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Autism is a neurodevelpmental disorder characterized by impaired verbal communication, limited reciprocal social interaction, restricted interests and repetitive behaviours. Twin and family studies indicate a large genetic contribution to ASDs (Autism Spectrum Disorders). During my Ph.D. I have been involved in several projects in which I used different genetic approaches in order to identify susceptibility genes in autism on chromosomes 2, 7 and X: 1)High-density SNP association and CNV analysis of two Autism Susceptibility Loci. The International Molecular Genetic Study of Autism Consortium (IMGSAC) previously identified linkage loci on chromosomes 7 and 2, termed AUTS1 and AUTS5, respectively. In this study, we evaluated the patterns of linkage disequilibrium (LD) and the distribution of haplotype blocks, utilising data from the HapMap project, across the two strongest peaks of linkage on chromosome 2 and 7. More than 3000 SNPs have been selected in each locus in all known genes, as well as SNPs in non-genic highly conserved sequences. All markers have been genotyped to perform a high-density association analysis and to explore copy number variation within these regions. The study sample consisted of 127 and 126 multiplex families, showing linkage to the AUTS1 and AUTS5 regions, respectively, and 188 gender-matched controls. Association and CNV analysis implicated several new genes, including IMMP2L and DOCK4 on chromosome 7 and ZNF533 and NOSTRIN on the chromosome 2. Particularly, my contribution to this project focused on the characterization of the best candidate gene in each locus: On the AUTS5 locus I carried out a transcript study of ZNF533 in different human tissues to verify which isoforms and start exons were expressed. High transcript variability and a new exon, never described before, has been identified in this analysis. Furthermore, I selected 31 probands for the risk haplotype and performed a mutation screen of all known exons in order to identify novel coding variants associated to autism. On the AUTS1 locus a duplication was detected in one multiplex family that was transmitted from father to an affected son. This duplication interrupts two genes: IMMP2L and DOCK4 and warranted further analysis. Thus, I performed a screening of the cohort of IMGSAC collection (285 multiplex families), using a QMPSF assay (Quantitative Multiplex PCR of Short fluorescent Fragments) to analyse if CNVs in this genic region segregate with autism phenotype and compare their frequency with a sample of 475 UK controls. Evidence for a role of DOCK4 in autism susceptibility was supported by independent replication of association at rs2217262 and the finding of a deletion segregating in a sib-pair family. 2)Analysis of X chromosome inactivation. Skewed X chromosome inactivation (XCI) is observed in females carrying gene mutations involved in several X-linked syndromes. We aimed to estimate the role of X-linked genes in ASD susceptibility by ascertaining the XCI pattern in a sample of 543 informative mothers of children with ASD and in a sample of 164 affected girls. The study sample included families from different european consortia. I analysed the XCI inactivation pattern in a sample of italian mothers from singletons families with ASD and also a control groups (144 adult females and 40 young females). We observed no significant excess of skewed XCI in families with ASD. Interestingly, two mothers and one girl carrying known mutations in X-linked genes (NLGN3, ATRX, MECP2) showed highly skewed XCI, suggesting that ascertainment of XCI could reveal families with X-linked mutations. Linkage analysis was carried out in the subgroup of multiplex families with skewed XCI (≥80:20) and a modest increased allele sharing was obtained in the Xq27-Xq28 region, with a peak Z score of 1.75 close to rs719489. In this region FMR1 and MECP2 have been associated in some cases with austim and therefore represent candidates for the disorder. I performed a mutation screen of MECP2 in 33 unrelated probands from IMGSAC and italian families, showing XCI skewness. Recently, Xq28 duplications including MECP2, have been identified in families with MR, with asymptomatic carrier females showing extreme (>85%) skewing of XCI. For these reason I used the sample of probands from X-skewed families to perform CNV analysis by Real-time quantitative PCR. No duplications have been found in our sample. I have also confirmed all data using as alternative method the MLPA assay (Multiplex Ligation dependent Probe Amplification). 3)ASMT as functional candidate gene for autism. Recently, a possible involvement of the acetylserotonin O-methyltransferase (ASMT) gene in susceptibility to ASDs has been reported: mutation screening of the ASMT gene in 250 individuals from the PARIS collection revealed several rare variants with a likely functional role; Moreover, significant association was reported for two SNPs (rs4446909 and rs5989681) located in one of the two alternative promoters of the gene. To further investigate these findings, I carried out a replication study using a sample of 263 affected individuals from the IMGSAC collection and 390 control individuals. Several rare mutations were identified, including the splice site mutation IVS5+2T>C and the L326F substitution previously reported by Melke et al (2007), but the same rare variants have been found also in control individuals in our study. Interestingly, a new R319X stop mutation was found in a single autism proband of Italian origin and is absent from the entire control sample. Furthermore, no replication has been found in our case-control study typing the SNPs on the ASMT promoter B.
Resumo:
Objectives In diabetic and non diabetic patients with peripheral artery obstructive disease (PAOD), we sought to establish whether the vascular wall damage, the mature circulating endothelium and the "in situ" neoangiogenesis are related with each other. Design In the peripheral blood of diabetic patients suffering critical ischaemia associated with peripheral artery disease, low levels and poor function of circulating endothelial progenitor cells (EPCs) were observed. Moreover, circulating endothelial cells (CECs) have been described in different conditions of vascular injury. In this type of disorders, which are all characterized by endothelial damage, neoangiogenesis plays a key role. Materials In the study we recruited 22 diabetic and 16 non diabetic patients, all of them suffering PAOD and critical ischaemia; healthy subjects and multiorgan donors have also been considered like controls. Methods Histopathologic characterization was performed on arterial tissue samples under a light microscope. Flow cytofluorimetric analysis was used to quantify CECs in peripheral blood samples. "In situ" expression of the Vascular Endothelial Growth Factor (VEGF) and Metalloproteinase 9 (MMP-9) transcripts was quantified in a Real Time-PCR analysis. Circulating VEGF concentration was determined by an ELISA assay. Results Arterial wall from diabetic patients, compared with non diabetic subjects, revealed a higher incidence of serious lesions (60% vs 47%) and a lower number of capillaries (65% vs 87%). Mean number of CECs/ml was significantly increased in all patients, compared to healthy controls (p=0.001). Compared to healthy subjects, VEGF transcripts expression resulted significantly higher in diabetic patients and in all patients (p<0.05) and a similar result was obtained in the MMP-9 transcripts expression. Serum VEGF concentration was significantly increased in PAOD patients correlated with controls (p=0.0431). Conclusions Our study demonstrates that in all patients considered, probably, regressive phenomenons prevail on reparative ones, causing an inesorable and progressive degeneration of the vascular wall, worse by diabetes. The vascular damage can be monitored by determining CECs number and its severity and development are emphasized by the MMP-9 transcripts expression. The "in situ" VEGF increased expression seems to be the evidence of a parietal cells bid to induce local angiogenesis. This reparing mechanism could induce the EPCs mobilitation by means the release of VEGF from the arterial wall. The mechanism, however, is ineffective like demonstrated by the EPCs reduced number and activities observed in patients suffering PAOD and critical ischaemia.
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In the wide range of data that the nutrition subject offers to the historical observation, this investigation focuses on one of the functions that food serves in the social context: that is, to signify cultural identity. In this context, we will analyse the ways in which industrially produced pasta has come to its status as one of the symbolic forms of twentieth-century Italian food, contributing to a sense of social identity that forms part of the process of nation-building developed during the XX century. The nature of the relationship between pasta and Italian food is analysed for a period of almost a century (1886-1984) through a variety of different sources: government enquiries, cookery books, gastronomic guides and menus of official dinners. The assemblage of such documents in one study allows investigation of certain themes throughout a wide range of gastronomical cultures active within the national borders. In this way, links are made between the production, adoption, reception and dissemination of the ingredients and Italian Unification.This method has made it possible to restore one possible form of historical knowledge of twentieth-century gastronomy and of the experiences by which it was influenced.
Resumo:
Si tratta di uno studio osservazionale analitico di coorte prospettico volto a rilevare disfunzioni neuropsicologiche nei pazienti affetti da epilessia frontale notturna, attraverso una batteria di test che esplora i seguenti domini cognitivi: intelligenza generale, memoria, linguaggio, funzioni esecutive, attenzione, vigilanza, tempi di reazione, percezione della qualità della vita ed eventuale presenza di sintomi psichiatrici. Lo studio ha un follow up medio di 20 anni e riporta, per la prima volta in letteratura, lâevoluzione clinica dei soggetti che hanno avuto un esordio dellâepilessia in età evolutiva. Fino ad ora, lâepilessia frontale notturna è stata associata a disfunzioni cognitive nei soli casi di famiglie affette e nelle quali è stato possibile rilevare il difetto genetico. Questo studio ha rilevato la prevalenza di disturbi cognitivi e psichici in un campione di 24 soggetti affetti, mediante la somministrazione di una batteria di test specifica. I risultati sono stati analizzati con il programma statistico SPSS. Tutti i soggetti presentano abilità cognitive inferiori alla media in uno o più test ma il quoziente intellettivo risulta normale nei tre quarti del campione. Il ritardo mentale è più frequente e più grave nei soggetti idiopatici rispetto a quelli con alterazioni morfologiche frontali rilevate alla risonanza magnetica. Sono risultati più frequenti i disturbi della memoria, soprattutto quella a lungo termine e del linguaggio rispetto a quelli di tipo disesecutivo. Tutti i soggetti, che non hanno ottenuto un controllo delle crisi, manifestano una percezione della qualità della vita inferiore alla media. Eâ stata valutata lâinfluenza delle variabili cliniche (età di esordio dellâepilessia, frequenza e semeiologia delle crisi, durata della malattia e terapia antiepilettica), le anomalie elettroencefalografiche e le anomalie rilevate alla risonanza magnetica. Le variabili che sono in rapporto con un maggiore numero di disfunzioni neuropsicologiche sono: lâelevata frequenza di crisi allâesordio, lâassociazione con crisi in veglia, la presenza di crisi parziali secondariamente generalizzate e lâassunzione di una politerapia. I disturbi psichici prevalgono nei soggetti con anomalie elettroencefalografiche frontali sinistre. I dati neuropsicologici suggeriscono una disfunzione cognitiva prevalentemente fronto-temporale e, assieme ai dati clinici ed elettroencefalografici, sembrano confermare lâorigine mesiale e orbitale frontale delle anomalie epilettiche nellâepilessia frontale notturna.
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The present dissertation focuses on an unfinished project for the construction of an inland waterway between Padua and Venice, in northern Italy. The history of this channel is analysed in the context of the general debate for the development of a waterway network in the Padanian plain. The project of reconstructing and enlarging the existing ancient channels for the development of a modern river transport system was born at the beginning of the 20th century as an attempt to withstand the railway’s concurrency. The main project aimed at transforming the Po river and other small rivers and channels in a big waterway for the connection of the most important northern industrial cities with Venice’s harbour and the Adriatic sea. Even if the idea of restoring the historical channel between Padua and Venice arose at the end of the First World War, it was only during the years 50s that a new project was conceived and the waterway was included in a global project for the construction of a whole new channel from Venice to Milan. The new project, strongly supported by the local Christian Democratic Party, was managed for more than twenty years causing a huge expenditure of money. After a great investment by both the central State and the local bodies (more than 100 millions euro) the project was finally abandoned. This research reconstructs the historical process and the economical motivations that sustained that project until its failure. Moreover, with the aim of understanding the reasons and the differences of such a failure, the history of inland waterway transport in Italy is compared with contemporary developments in Germany.
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During the wake sleep (W-S) cycle in mammals, the alternation of the different states, wake, NREM sleep (NREMS) and REM sleep (REMS), is associated not only with electroencephalographic or behavioural changes, but also with modifications in the physiological regulations of the organism. The most evident change is the existence of a suspension of the somatic and autonomic thermoregulatory responses during REMS. Since thermoregulation is prevalently controlled by the Preoptic Area-Anterior Hypothalamus (PO-AH), its suspension during REM sleep has been taken as a sign of an impairment of the hypothalamic integrative activity that could explain the modifications in physiological regulation observed in this sleep stage. The recent finding from our laboratory that the secretion of the antidiuretic hormone arginine-vasopressin (AVP) in response to a central osmotic stimulation is quantitatively the same throughout the different stages of the W-S cycle, has shown that hypothalamic osmoregulation is not suspended during REMS. In order to clarify the extent of the hypothalamic involvement in the regulation of the W-S cycle, we have studied the effects of three days of water deprivation and of two days of recovery during which animals were allowed a free access to water, on the architecture of the W-S cycle. The condition of water deprivation represents a severe challenge involving neuroendocrine and autonomic hypothalamic regulations. In contradiction with thermoregulatory studies, in which it has been clearly demonstrated that a thermal challenge selectively reduces REMS occurrence, the results of this study show that REMS occurrence is mildly reduced only in the third day of water deprivation. The most striking effects produced by water deprivation appear to concern NREMS, which shows a selective and significant reduction in its slow EEG activity (delta-power) but not in its duration. The recovery period is mainly characterized by a disruption of the normal circadian rhythm of REMS occurrence and by a rebound of the delta power in NREMS. Thus, an autonomic challenge different from those related to thermoregulation and an endocrine challenge as the continuous secretion of AVP show to exert different effects on the stages of the wake-sleep cycle. Also, this study demonstrates that the impairment of the hypothalamic integrative activity thought to characterize the occurrence of REMS only involves thermoregulatory structures.
Resumo:
9-hydroxystearic acid (9-HSA) is an endogenous lipoperoxidation product and its administration to HT29, a colon adenocarcinoma cell line, induced a proliferative arrest in G0/G1 phase mediated by a direct activation of the p21WAF1 gene, bypassing p53. We have previously shown that 9-HSA controls cell growth and differentiation by inhibiting histone deacetylase 1 (HDAC1) activity, showing interesting features as a new anticancer drug. The interaction of 9-HSA with the catalytic site of the 3D model has been tested with a docking procedure: noticeably, when interacting with the site, the (R)-9-enantiomer is more stable than the (S) one. Thus, in this study, (R)- and (S)-9-HSA were synthesized and their biological activity tested in HT29 cells. At the concentration of 50 M (R)-9-HSA showed a stronger antiproliferative effect than the (S) isomer, as indicated by the growth arrest in G0/G1. The inhibitory effect of (S)-9-HSA on HDAC1, HDAC2 and HDAC3 activity was less effective than that of the (R)-9-HSA in vitro, and the inhibitory activity of both the (R)- and the (S)-9-HSA isomer, was higher on HDAC1 compared to HDAC2 and HDAC3, thus demonstrating the stereospecific and selective interaction of 9-HSA with HDAC1. In addition, histone hyperacetylation caused by 9-HSA treatment was examined by an innovative HPLC/ESI/MS method. Analysis on histones isolated from control and treated HT29 confirmed the higher potency of (R)-9-HSA compared to (S)-9-HSA, severely affecting H2A-2 and H4 acetylation. On the other side, it seemed of interest to determine whether the G0/G1 arrest of HT29 cell proliferation could be bypassed by the stimulation with the growth factor EGF. Our results showed that 9-HSA-treated cells were not only prevented from proliferating, but also showed a decreased [3H]thymidine incorporation after EGF stimulation. In this condition, HT29 cells expressed very low levels of cyclin D1, that didn’t colocalize with HDAC1. These results suggested that the cyclin D1/HDAC1 complex is required for proliferation. Furthermore, in the effort of understanding the possible mechanisms of this effect, we have analyzed the degree of internalization of the EGF/EGFR complex and its interactions with HDAC1. EGF/EGFR/HDAC1 complex quantitatively increases in 9-HSA-treated cells but not in serum starved cells after EGF stimulation. Our data suggested that 9-HSA interaction with the catalytic site of the HDAC1 disrupts the HDAC1/cyclin D1 complex and favors EGF/EGFR recruitment by HDAC1, thus enhancing 9-HSA antiproliferative effects. In conclusion 9-HSA is a promising HDAC inhibitor with high selectivity and specificity, capable of inducing cell cycle arrest and histone hyperacetylation, but also able to modulate HDAC1 protein interaction. All these aspects may contribute to the potency of this new antitumor agent.
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“Naturally occurring cancers in pet dogs and humans share many features, including histological appearance, tumour genetics, molecular targets, biological behaviour and response to conventional therapies. Studying dogs with cancer is likely to provide a valuable perspective that is distinct from that generated by the study of human or rodent cancers alone. The value of this opportunity has been increasingly recognized in the field of cancer research for the identification of cancer-associated genes, the study of environmental risk factors, understanding tumour biology and progression, and, perhaps most importantly, the evaluation and development of novel cancer therapeutics”.(Paoloni and Khanna, 2008) In last years, the author has investigated some molecular features of cancer in dogs. The Thesis is articulated in two main sections. In section 1, the preliminary results of a research project aimed at investigating the role of somatic mutations of Ataxia-Telangiectasia mutated (ATM) gene in predisposing to cancer in boxer dogs, are presented. The canine boxer breed may be considered an unique opportunity to disclose the role of ATM somatic mutation since boxer dogs are known to be dramatically susceptible to cancer and since they may be considered a closed gene pool. Furthermore, dogs share with human the some environment. Overall, the abovementioned features could be considered extremely useful for our purposes. In the section 2, the results of our studies aimed at setting up accurate and sensitive molecular assays for diagnosing and assessing minimal residual disease in lymphoproliferative disorders of dogs, are presented. The results of those molecular assay may be directly translated in the field of Veterinary practice as well as the may be used to improve our objective evaluation of new investigational drugs effectiveness in canine cancer trials.
Resumo:
L’Azienda USL di Bologna è la più grande della regione ed è una delle più grandi in Italia: serve una popolazione di 836.697 abitanti ed è distribuita su 50 comuni. E’ stata istituita il 1° gennaio 2004 con la Legge della Regione Emilia Romagna n. 21 del 20/10/2003 che ha unificato i Comuni di tre Aziende USL: “Città di Bologna”, “Bologna Sud” e “Bologna Nord” (ad eccezione del Comune di Medicina che dall’Area Nord è entrato a far parte dell’Azienda USL di Imola che ha mantenuto un’autonoma configurazione giuridica). Il territorio dell’Azienda USL di Bologna si estende per 2915,4 Kmq ed è caratterizzato dalla particolare ubicazione geografica dei suoi distretti. Al Distretto prettamente urbano, quale quello di Bologna Città si affiancano nell’Area Nord i Distretti di pianura quali Pianura Est e Pianura Ovest, mentre nell’Area Sud si collocano i Distretti con territorio più collinare, quali quelli di Casalecchio di Reno e San Lazzaro di Savena ed il Distretto di Porretta Terme che si caratterizza per l’alta percentuale di territorio montuoso. L’unificazione di territori diversi per caratteristiche orografiche, demografiche e socioeconomiche, ha comportato una maggiore complessità rispetto al passato in termini di governo delle condizioni di equità. La rimodulazione istituzionale ed organizzativa dell’offerta dei sevizi sanitari ha comportato il gravoso compito di razionalizzarne la distribuzione, tenendo conto delle peculiarità del contesto. Alcuni studi di fattibilità precedenti l’unificazione, avevano rilevato come attraverso la costituzione di un’Azienda USL unica si sarebbero potuti più agevolmente perseguire gli obiettivi collegati alle prospettive di sviluppo e di ulteriore qualificazione del sistema dei servizi delle Aziende USL dell’area bolognese, con benefici per il complessivo servizio sanitario regionale. Le tre Aziende precedentemente operanti nell’area bolognese erano percepite come inadeguate, per dimensioni, a supportare uno sviluppo dei servizi ritenuto indispensabile per la popolazione ma, che, se singolarmente realizzato, avrebbe condotto ad una inutile duplicazione di servizi già presenti. Attraverso l’integrazione delle attività di acquisizione dei fattori produttivi e di gestione dei servizi delle tre Aziende, si sarebbero potute ragionevolmente conseguire economie più consistenti rispetto a quanto in precedenza ottenuto attraverso il coordinamento volontario di tali processi da parte delle tre Direzioni. L’istituzione della nuova Azienda unica, conformemente al Piano sanitario regionale si proponeva di: o accelerare i processi di integrazione e di redistribuzione dell’offerta dei servizi territoriali, tenendo conto della progressiva divaricazione fra i cambiamenti demografici, che segnavano un crescente deflusso dal centro storico verso le periferie, ed i flussi legati alle attività lavorative, che si muovevano in senso contrario; o riorganizzare i servizi sanitari in una logica di rete e di sistema, condizione necessaria per assicurare l’equità di accesso ai servizi e alle cure, in stretta interlocuzione con gli Enti Locali titolari dei servizi sociali; o favorire il raggiungimento dell’equilibrio finanziario dell’Azienda e contribuire in modo significativo alla sostenibilità finanziaria dell’intero sistema sanitario regionale. L’entità delle risorse impegnate nell’Area bolognese e le dimensioni del bilancio della nuova Azienda unificata offrivano la possibilità di realizzare economie di scala e di scopo, attraverso la concentrazione e/o la creazione di sinergie fra funzioni e attività, sia in ambito ospedaliero, sia territoriale, con un chiaro effetto sull’equilibrio del bilancio dell’intero Servizio sanitario regionale. A cinque anni dalla sua costituzione, l’Azienda USL di Bologna, ha completato una significativa fase del complessivo processo riorganizzativo superando le principali difficoltà dovute alla fusione di tre Aziende diverse, non solo per collocazione geografica e sistemi di gestione, ma anche per la cultura dei propri componenti. La tesi affronta il tema dell’analisi dell’impatto della fusione sugli assetti organizzativi aziendali attraverso uno sviluppo così articolato: o la sistematizzazione delle principali teorie e modelli organizzativi con particolare attenzione alla loro contestualizzazione nella realtà delle organizzazioni professionali di tipo sanitario; o l’analisi principali aspetti della complessità del sistema tecnico, sociale, culturale e valoriale delle organizzazioni sanitarie; o l’esame dello sviluppo organizzativo dell’Azienda USL di Bologna attraverso la lettura combinata dell’Atto e del Regolamento Organizzativo Aziendali esaminati alla luce della normativa vigente, con particolare attenzione all’articolazione distrettuale e all’organizzazione Dipartimentale per cogliere gli aspetti di specificità che hanno caratterizzano il disegno organizzativo globalmente declinato. o l’esposizione degli esiti di un questionario progettato, in accordo con la Direzione Sanitaria Aziendale, allo scopo di raccogliere significativi elementi per valutare l’impatto della riorganizzazione dipartimentale rispetto ai tre ruoli designati in “staff “alle Direzioni degli otto Dipartimenti Ospedalieri dell’AUSL di Bologna, a tre anni dalla loro formale istituzione. La raccolta dei dati è stata attuata tramite la somministrazione diretta, ai soggetti indagati, di un questionario costituito da numerosi quesiti a risposta chiusa, integrati da domande aperte finalizzate all’approfondimento delle dimensioni di ruolo che più frequentemente possono presentare aspetti di criticità. Il progetto ha previsto la rielaborazione aggregata dei dati e la diffusione degli esiti della ricerca: alla Direzione Sanitaria Aziendale, alle Direzioni Dipartimentali ospedaliere ed a tutti i soggetti coinvolti nell’indagine stessa per poi riesaminare in una discussione allargata i temi di maggiore interesse e le criticità emersi. Gli esiti sono esposti in una serie di tabelle con i principali indicatori e vengono adeguatamente illustrati.
